Separate Gut Plasma Cell Populations Produce Auto‐Antibodies against Transglutaminase 2 and Transglutaminase 3 in Dermatitis Herpetiformis

Das, Saykat; Stamnæs, Jorunn; Kemppainen, Esko; Hervonen, Kaisa; Lundin, Knut E.A.; Parmar, Naveen; Jahnsen, Frode L.; Jahnsen, Jørgen; Lindfors, Katri; Salmi, Teea; Iversen, Rasmus; Sollid, Ludvig M.

doi:10.1002/advs.202300401

Advanced Science

2023

DOI: 10.1002/advs.202300401

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Separate Gut Plasma Cell Populations Produce Auto‐Antibodies against Transglutaminase 2 and Transglutaminase 3 in Dermatitis Herpetiformis

Saykat Das

Jorunn Stamnæs

Esko Kemppainen

et al.

Abstract: Dermatitis herpetiformis (DH) is an inflammatory skin disorder often considered as an extra intestinal manifestation of celiac disease (CeD). Hallmarks of CeD and DH are auto‐antibodies to transglutaminase 2 (TG2) and transglutaminase 3 (TG3), respectively. DH patients have auto‐antibodies reactive with both transglutaminase enzymes. Here it is reported that in DH both gut plasma cells and serum auto‐antibodies are specific for either TG2 or TG3 with no TG2–TG3 cross reactivity. By generating monoclonal antibo… Show more

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Cited by 3 publications

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Autoantibody binding and unique enzyme-substrate intermediate conformation of human transglutaminase 3

Heggelund,

Das,

Stamnaes

et al. 2023

Nat Commun

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Transglutaminase 3 (TG3), the autoantigen of dermatitis herpetiformis (DH), is a calcium dependent enzyme that targets glutamine residues in polypeptides for either transamidation or deamidation modifications. To become catalytically active TG3 requires proteolytic cleavage between the core domain and two C-terminal β-barrels (C1C2). Here, we report four X-ray crystal structures representing inactive and active conformations of human TG3 in complex with a TG3-specific Fab fragment of a DH patient derived antibody. We demonstrate that cleaved TG3, upon binding of a substrate-mimicking inhibitor, undergoes a large conformational change as a β-sheet in the catalytic core domain moves and C1C2 detaches. The unique enzyme-substrate conformation of TG3 without C1C2 is recognized by DH autoantibodies. The findings support a model where B-cell receptors of TG3-specific B cells bind and internalize TG3-gluten enzyme-substrate complexes thereby facilitating gluten-antigen presentation, T-cell help and autoantibody production.

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Autoantibody binding and unique enzyme-substrate intermediate conformation of human transglutaminase 3

Heggelund,

Das,

Stamnaes

et al. 2023

Nat Commun

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Cerebellar degeneration in gluten ataxia is linked to microglial activation

Floare,

Wharton,

Simpson

et al. 2024

Brain Communications

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Gluten sensitivity has long been recognised exclusively for its gastrointestinal involvement, however more recent research provides evidence for the existence of neurological manifestations that can appear in combination with, or independent of the small bowel manifestations. Amongst all neurological manifestations of gluten sensitivity, Gluten ataxia is the most commonly occurring one, accounting for up to 40% of cases of idiopathic sporadic ataxia. However, despite its prevalence, its neuropathological basis is still poorly defined. Here we provide a neuropathological characterisation of gluten ataxia and compare the presence of neuroinflammatory markers GFAP, Iba-1, MHC-II and CD68 in the central nervous system of 4 gluten ataxia cases to 5 ataxia controls and 7 neurologically healthy controls. Our results demonstrate that severe cerebellar atrophy, CD20+ and CD8+ lymphocytic infiltration in the cerebellar grey and white matter and a significant upregulation of microglial immune activation in the cerebellar granular layer, molecular layer, and cerebellar white matter are features of Gluten ataxia, providing evidence for the involvement of both cellular and humoral immune-mediated processes in gluten ataxia pathogenesis.

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Coeliac disease: the paradox of diagnosing a food hypersensitivity disorder with autoantibodies

du Pre,

Iversen,

Sollid

2024

Gut

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Serum antibodies to the autoantigen transglutaminase 2 (TG2) are increasingly harnessed to diagnose coeliac disease. Diagnostic guidelines for children give recommendation for a no-biopsy-based diagnosis through detection of high amounts of IgA anti-TG2 antibodies in serum with confirmation of positivity in a separate blood sample by characteristic autoantibody-staining of tissue. While measurement of IgA anti-TG2 also is important in the diagnostic workup of adults, the adult guidelines still mandate examination of gut biopsies. This requirement might well change in the future, as might the necessity for confirming autoantibody positivity by tissue staining. The key role of autoantibody serology for diagnosis of coeliac disease is paradoxical. Coeliac disease was considered, and still can be considered, a food intolerance disorder where autoantibodies at face value are out of place. The immunological mechanisms underlying the formation of autoantibodies in response to gluten exposure have been dissected. This review presents the current insights demonstrating that the autoantibodies in coeliac disease are intimately integrated in the maladapted immune response to gluten.

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Separate Gut Plasma Cell Populations Produce Auto‐Antibodies against Transglutaminase 2 and Transglutaminase 3 in Dermatitis Herpetiformis

Cited by 3 publications

References 50 publications

Autoantibody binding and unique enzyme-substrate intermediate conformation of human transglutaminase 3

Autoantibody binding and unique enzyme-substrate intermediate conformation of human transglutaminase 3

Cerebellar degeneration in gluten ataxia is linked to microglial activation

Coeliac disease: the paradox of diagnosing a food hypersensitivity disorder with autoantibodies

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